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[器质性非精神病性障碍中的炎症标志物]

[Inflammatory markers in organic nonpsychotic disorders].

作者信息

Androsova L V, Vetlugina T P, Nikitina V B, Zozulya S A, Otman I N, Belokrylova M F, Klyushnik T P

机构信息

Mental Health Research Centre, Moscow, Russia.

Mental Health Research Institute - Tomsk National Research Medical Center Russian Academy of Sciences, Tomsk, Russia.

出版信息

Zh Nevrol Psikhiatr Im S S Korsakova. 2023;123(3):88-93. doi: 10.17116/jnevro202312303188.

Abstract

OBJECTIVE

To determine the indicators of systemic inflammation in peripheral blood samples of patients with organic non-psychotic disorders.

MATERIAL AND METHODS

The study included 60 patients, aged 56.9±7.7 years, with a disease duration of 7.3±5.55 years, with a verified ICD-10 diagnosis «Organic emotionally labile (asthenic) disorder» (F06.6) and «Organic Anxiety Disorder» (F06.4). Patients with organic asthenic disorder were divided into two groups according to the prevailing symptoms: 36 patients with asthenic-cephalgic syndrome (AC); 10 patients with astheno-dysthymic syndrome (AD); the third group (=14) included patients with organic anxiety disorder (AND). The control group consisted of 65 people matched for age and sex with patients. The activity of leukocyte elastase (LE) and α1-proteinase inhibitor (α1-PI) was determined by the spectrophotometric method, the levels of aAB to S100b and MBP were determined by ELISA. The protease-inhibitory index (PII), i.e., the ratio of LE activity to α1-PI, was calculated.

RESULTS

A significant increase in LE (235.4 [216.4; 258.1] nmol/min*ml, <0.001), the functional activity of α1-PI (43.1 [38.7; 47.6] u/ml, <0.001), the level of aAB to S100b (0.78 [0.70; 0.89] opt.units, <0.05) and a decrease in PII (6.19 [5.32; 6.9], <0.05) in the group of patients with organic non-mental disorders compared with controls were shown. Deviations from the normal values of immune markers of inflammation in blood samples were also found in various syndromes. Clustering of the total group of patients by LE activity made it possible to identify 2 immunotypes with a balanced and unbalanced inflammatory process, confirming the clinical diversity of the disease: 60% of patients with AC syndrome belong to the 1st cluster, in which the ratio of immune markers characterizes a balanced inflammatory process aimed at restoration of homeostasis; 80% of patients with organic AND belong to the second cluster, which characterizes low proteolytic activity and imbalance of inflammation, which is an unfavorable prognostic factor in terms of the further course of the disease and therapy.

CONCLUSION

The results confirm the importance of the inflammatory link in the neuroprogression of organic non-psychotic disorders. The identified features of the immune response can serve as an additional paraclinical criterion for differential diagnosis and evaluation of the prognosis of the further development of the disease.

摘要

目的

确定器质性非精神病性障碍患者外周血样本中的全身炎症指标。

材料与方法

该研究纳入了60例患者,年龄为56.9±7.7岁,病程为7.3±5.55年,经核实的ICD - 10诊断为“器质性情绪不稳定(虚弱)障碍”(F06.6)和“器质性焦虑障碍”(F06.4)。患有器质性虚弱障碍的患者根据主要症状分为两组:36例患有虚弱 - 头痛综合征(AC);10例患有虚弱 - 心境恶劣综合征(AD);第三组(=14例)包括患有器质性焦虑障碍(AND)的患者。对照组由65名年龄和性别与患者匹配的人组成。采用分光光度法测定白细胞弹性蛋白酶(LE)和α1 - 蛋白酶抑制剂(α1 - PI)的活性,采用酶联免疫吸附测定法测定抗S100b和髓鞘碱性蛋白(MBP)的抗体水平。计算蛋白酶抑制指数(PII),即LE活性与α1 - PI的比值。

结果

与对照组相比,器质性非精神障碍患者组的LE显著升高(235.4 [216.4; 258.1] nmol/min*ml,<0.001),α1 - PI的功能活性升高(43.1 [38.7; 47.6] u/ml,<0.001),抗S100b抗体水平升高(0.78 [0.70; 0.89] opt.units,<0.05),PII降低(6.19 [5.32; 6.9],<0.05)。在各种综合征中也发现了血液样本中炎症免疫标志物偏离正常值的情况。通过LE活性对患者总群体进行聚类分析,能够识别出2种免疫类型,其炎症过程平衡和不平衡,证实了该疾病的临床多样性:60%的AC综合征患者属于第一类聚类,其中免疫标志物的比值表征了旨在恢复内环境稳态的平衡炎症过程;80%的器质性AND患者属于第二类聚类,其特征为低蛋白水解活性和炎症失衡,就疾病的进一步发展和治疗而言,这是一个不利的预后因素。

结论

结果证实了炎症环节在器质性非精神病性障碍神经进展中的重要性。所确定的免疫反应特征可作为鉴别诊断和评估疾病进一步发展预后的额外辅助临床标准。

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